Platelet-Rich Plasma: The Science of Dosing and Healing
Table of Contents
As a clinician and researcher dedicated to integrative and functional medicine, I am constantly exploring the most effective, evidence-based treatments for my patients. Platelet-Rich Plasma (PRP) therapy stands out as a powerful tool in regenerative medicine, particularly for musculoskeletal conditions. However, not all PRP is created equal. In this educational post, I will take you on a journey through the intricate world of PRP, drawing from the latest findings of leading researchers. We will explore the fundamental biology of platelets, dissect the critical importance of PRP dosing and formulation, and examine how factors such as age and the presence of other cells, including white blood cells, can dramatically influence treatment outcomes. I will also explain how we calculate and customize these treatments in a clinical setting, and how integrating these advanced biological therapies with foundational care, such as integrative chiropractic, can optimize healing and provide a comprehensive path to recovery.
To truly appreciate the power of PRP therapy, we first need to revisit a fundamental concept from our early medical training: the platelet. These are not complete cells but rather tiny, anucleated (lacking a nucleus) cell fragments that circulate in our blood. Despite their small size, they are biological powerhouses, densely packed with hundreds of proteins, growth factors, and cytokines essential for healing.
Platelets have a relatively short lifespan of about seven to ten days. This is a crucial piece of information, especially when I advise patients to restrict the use of non-steroidal anti-inflammatory drugs (NSAIDs) before a procedure, as these medications can interfere with platelet function.
In a healthy individual, the typical platelet count ranges from 150,000 to 400,000 per microliter of blood. The FDA’s definition of PRP is somewhat broad, simply stating it’s a concentration of platelets above this normal baseline. Our goal with PRP therapy is to harness the body’s innate healing capacity by concentrating these vital platelets and their associated growth factors and then delivering this potent biological product precisely to an area of injury or degeneration. This targeted delivery initiates and amplifies the body’s natural healing cascade.
While the concept of PRP is straightforward, the execution is anything but. There is significant variability among commercially available systems for preparing PRP, which can lead to markedly different clinical outcomes. This isn’t just a minor detail; it’s at the core of whether a treatment succeeds or fails.
A pivotal study from Australia by James and colleagues (2016) examined five different commercial PRP systems and found dramatic differences in both the final platelet concentration and the number of white blood cells included in the final product. Imagine the same patient’s blood being processed through four different systems. The resulting PRP can range in color from light straw-yellow to deep red, each color representing a different cellular composition. This “rainbow” of PRP products highlights the lack of standardization in the field.
This variability has significant implications for our evaluation of the scientific evidence. For years, colleagues and patients have asked about the evidence supporting PRP. A landmark meta-analysis by Meheux et al. (2016) revealed something fascinating: more patients have been enrolled in clinical trials for PRP for knee osteoarthritis (OA) than for other common treatments like hyaluronic acid injections. The data exists, but the variability in results often stems from the variability in the PRP product used. Generally, high-quality studies show that PRP therapy tends to outperform hyaluronic acid in the medium- to long-term.
So, how do we create this biologic therapy? The process begins with a simple blood draw right here in the office. The amount of blood we draw is a critical first step—less blood means fewer total platelets to start with, while a larger volume gives us more raw material to create a higher-dose product.
Understanding the specific mechanics of your chosen system is paramount to maximizing the therapeutic potential of the PRP you deliver to your patients.
Although the FDA doesn’t regulate PRP as a drug with specific dosage requirements, we must consider it a biologic drug. Like any medication, there is a therapeutic dose-response curve. A dose that is too low (subtherapeutic) will fail to produce a biological effect, while an excessively high dose can, in some cases, have an inhibitory or even detrimental effect.
Research has begun to clarify what these therapeutic doses might be. For tendon injuries, studies have shown an optimal platelet concentration that best stimulates tenocyte (tendon cell) regeneration. As you go above that optimal concentration, you can actually see a decrease in tenocyte proliferation (Giusti et al., 2009). This highlights that simply aiming for the highest possible concentration isn’t the right strategy.
So, what is the right clinical dose? The answer varies by the tissue we are treating. A groundbreaking study by Peter Everts’ group examined various soft-tissue applications of PRP (Everts et al., 2020). They meticulously calculated the total platelet dose administered in numerous published studies and correlated it with clinical outcomes.
The results were striking. They found a clear threshold. Studies with total platelet doses below 3.5 billion platelets were overwhelmingly negative. In contrast, studies using a dose above 3.5 billion platelets were predominantly positive. This suggests a therapeutic threshold for soft tissue applications. If your PRP system can only produce, say, 1.5 billion platelets from a standard blood draw, you may be consistently under-dosing your patients and seeing disappointing results.
Further research from Scott Rodeo’s group at the Hospital for Special Surgery reinforced this dose-dependent effect, showing that studies using higher-dose PRP reported significantly better outcomes (Cole et al., 2021). The emerging consensus is that for many soft-tissue and tendon injuries, a platelet dose of 3.5 to 10 billion platelets is likely necessary to achieve a robust clinical effect.
Another critical factor we must consider is the patient’s age. As we age, the regenerative capacity of our cells can decline. Emerging evidence suggests that older patients may require a higher total dose of PRP to achieve the same therapeutic effect as a younger patient. In my clinical practice, this means I might opt for a larger initial blood draw for an older individual to ensure we can generate a sufficiently potent PRP product. We are still in the early stages of understanding these nuances, but personalizing treatment based on patient factors such as age is a cornerstone of effective biologic therapy.
Knee osteoarthritis (OA) is one of the most-studied applications for PRP, and it provides an excellent case study in the importance of dosing. The well-known RESTORE trial, published in JAMA, initially concluded that PRP was not effective for knee OA (Bennell et al., 2021). However, when you dig into the methodology, you find the issue: they used a low-dose PRP system that delivered only 1.6 billion platelets per injection. Based on our dose-response curve, this is a subtherapeutic dose, so a negative result is not surprising. While the study was impeccably conducted, it taught us a valuable lesson about the importance of using an adequate biologic dose.
In stark contrast, another widely cited study used a much higher dose of 10 billion platelets (Bansal et al., 2021). In this high-dose trial, patients not only experienced significant improvements in pain and function, but imaging studies also showed a slowing of cartilage degeneration. This suggests a potential disease-modifying effect—something we rarely see with other treatments. Other studies have found similar benefits with repeated injections totaling 5 to 15 billion platelets. For knee OA, the therapeutic target appears to be in the 5-10 billion platelet range.
In the literature and among clinicians, you’ll often hear PRP described by its concentration, such as “2x, 3x, or 4x” baseline. This can be misleading. Imagine you have 5 billion platelets in a glass. That is your total dose. Now, if you add a lot of water (plasma), the concentration goes down, but the total number of platelets remains the same. Conversely, if you remove most of the water, the concentration increases, but the dose remains 5 billion.
I advocate for discussing and studying PRP in terms of total platelet dose (the absolute number of platelets being injected) rather than concentration. The total dose is a more accurate and reproducible measure of the biological substance being delivered. To calculate this in the clinic, you need two things: the patient’s baseline platelet count (from a CBC) and the recovery efficiency of your specific PRP system. While a baseline CBC can fluctuate, it provides a crucial starting point for individualizing treatment and ensuring we are meeting our therapeutic target.
Platelets are not the only cells in the PRP mixture. The “buffy coat” also contains a significant number of leukocytes, or white blood cells (WBCs). This has led to a major debate in the field: is it better to use leukocyte-rich (LR-PRP) or leukocyte-poor (LP-PRP) formulations?
The data comparing LR-PRP and LP-PRP is mixed. Some studies, particularly those from outside Europe, suggest that for knee OA, there may not be a significant clinical difference in long-term outcomes, although LR-PRP often causes greater initial inflammation. My approach is to consider the injection site and the underlying pathology. For an intra-articular injection (inside a joint), I often lean towards an LP-PRP formulation to minimize the initial inflammatory flare. For a tendon injury, where a robust inflammatory signal is needed to jump-start a chronic, stagnant healing process, a leukocyte-rich formulation may be more appropriate.
PRP therapy is a powerful tool, but it is not a magic bullet. To achieve the best possible outcomes, it must be integrated into a comprehensive rehabilitation plan. This is where the principles of integrative chiropractic care become indispensable.
The goal of a PRP injection is to create a biological scaffold (a clot rich in growth factors) directly at the site of tissue damage, thereby initiating a healing response. Ultrasound guidance is non-negotiable for this; we must ensure we are delivering the product precisely into the tendon tear or joint space. If the injection is off-target, the therapy will fail.
Following the procedure, the body needs the right environment to heal. This involves:
This integrative approach, combining advanced biologic therapies like precisely dosed PRP with foundational chiropractic care and rehabilitation, addresses both the biological deficit and the biomechanical dysfunction, leading to more complete and durable outcomes for my patients. The big takeaway is that true success in regenerative medicine comes from a deep understanding of the biologic product you are delivering and integrating it into a holistic, patient-centered treatment plan.
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The information herein on "Platelet-Rich Plasma: The Science of Dosing and Healing" is not intended to replace a one-on-one relationship with a qualified health care professional or licensed physician and is not medical advice. We encourage you to make healthcare decisions based on your research and partnership with a qualified healthcare professional.
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Dr. Alex Jimenez DC, MSACP, APRN, FNP-BC*, CCST, IFMCP, CFMP, ATN
email: coach@elpasofunctionalmedicine.com
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Licensed as a Doctor of Chiropractic (DC) in Texas & New Mexico*
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ANCC FNP-BC: Board Certified Nurse Practitioner*
Compact Status: Multi-State License: Authorized to Practice in 40 States*
Graduate with Honors: ICHS: MSN-FNP (Family Nurse Practitioner Program)
Degree Granted. Master's in Family Practice MSN Diploma (Cum Laude)
Dr. Alex Jimenez, DC, APRN, FNP-BC*, CFMP, IFMCP, ATN, CCST
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Licenses and Board Certifications:
DC: Doctor of Chiropractic
APRNP: Advanced Practice Registered Nurse
FNP-BC: Family Practice Specialization (Multi-State Board Certified)
RN: Registered Nurse (Multi-State Compact License)
CFMP: Certified Functional Medicine Provider
MSN-FNP: Master of Science in Family Practice Medicine
MSACP: Master of Science in Advanced Clinical Practice
IFMCP: Institute of Functional Medicine
CCST: Certified Chiropractic Spinal Trauma
ATN: Advanced Translational Neutrogenomics
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TCA: Texas Chiropractic Association: Member ID: 104311
AANP: American Association of Nurse Practitioners: Member ID: 2198960
ANA: American Nurse Association: Member ID: 06458222 (District TX01)
TNA: Texas Nurse Association: Member ID: 06458222
NPI: 1205907805
| Primary Taxonomy | Selected Taxonomy | State | License Number |
|---|---|---|---|
| No | 111N00000X - Chiropractor | NM | DC2182 |
| Yes | 111N00000X - Chiropractor | TX | DC5807 |
| Yes | 363LF0000X - Nurse Practitioner - Family | TX | 1191402 |
| Yes | 363LF0000X - Nurse Practitioner - Family | FL | 11043890 |
| Yes | 363LF0000X - Nurse Practitioner - Family | CO | C-APN.0105610-C-NP |
| Yes | 363LF0000X - Nurse Practitioner - Family | NY | N25929 |
Dr. Alex Jimenez, DC, APRN, FNP-BC*, CFMP, IFMCP, ATN, CCST
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